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首页> 外文期刊>Magnetic resonance imaging: An International journal of basic research and clinical applications >Analysis of pharmacokinetics of Gd-DTPA for dynamic contrast-enhanced magnetic resonance imaging
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Analysis of pharmacokinetics of Gd-DTPA for dynamic contrast-enhanced magnetic resonance imaging

机译:动态对比增强磁共振成像Gd-DTPA药代动力学分析

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摘要

The pharmacokinetics (PK) of the contrast agent Gd-DTPA administered intravenously (i.v.) for contrast-enhanced MR imaging (DCE-MRI) is an important factor for quantitative data acquisition. We studied the effect of various initial bolus doses on the PK of Gd-DTPA and analyzed population PK of a lower dose for intra-subject variations in DCE-MRI. First, fifteen subjects (23-85 years, M/F) were randomly divided into four groups for DCE-MRI with different Gd-DTPA dose: group-I, 0.1 mmol/kg, n = 4; group-II, 0.05 mmol/kg, n = 4; group-III, 0.025 mmol/kg, n = 4; and group-IV, 0.0125 mmol/kg, n = 3. Sequential fast T1 mapping sequence, after a bolus i.v. Gd-DTPA administered, and a linear T1-[Gd-DTPA] relationship were used to estimate the PK of Gd-DTPA. Secondly, MR-acquired PKs of Gd-DTPA from 58 subjects (2880 years, M/F) were collected retrospectively, from an ongoing study of the brain using DCE-MRI with Gd-DTPA at 0.025 mmol/kg, to statistically analyze population PK of Gd-DTPA. We found that the PK of Gd-DTPA (i.v. 0.025 mmol/kg) had a half-life of 37.3 +/- 6.6 min, and was a better fit into a linear T1-[Gd-DTPA] relationship than higher doses (up to 0.1 mmol/kg). The area under the curve (AUC) for 0.025 mmol/kg was 337 +/- 0.46, which was a quarter of AUC of 0.1 mmol/kg. In population analysis, a dose of 0.025 mmol/kg of Gd-DTPA provided less than 5% subject-dependent variation in the PK of Gd-DTPA. Administration of 0.025 mmol/kg Gd-DTPA enabled us to estimate [Gd-DTPA] from T1 by using a linear relationship that has a lower estimation error compared to a non-linear relationship. DCE-MRI with a quarter dose of Gd-DTPA is more sensitive to detect changes in [Gd-DTPA]. (C) 2016 Elsevier Inc. All rights reserved.
机译:触摸剂GD-DTPA的药代动力学(PK)静脉内(I.V.)用于对比增强的MR成像(DCE-MRI)是定量数据采集的重要因素。我们研究了各种初始推注剂量对GD-DTPA的PK的影响,并分析了DCE-MRI中对象内含量的较低剂量的群体PK。首先,将十五个受试者(23-85岁,M / F)随机分为四组的DCE-MRI,具有不同的GD-DTPA剂量:基团-I,0.1mmol / kg,n = 4; -II,0.05mmol / kg,n = 4; -III组,0.025mmol / kg,n = 4;和第四组,0.0125mmol / kg,n = 3.顺序快速T1映射序列,在推杆之后。施用GD-DTPA,并且使用线性T1- [GD-DTPA]关系来估计GD-DTPA的PK。其次,回顾性地收集来自58个受试者(2880岁,M / F)的GD-DTPA的先生PKS,从使用DCE-MRI与0.025mmol / kg的DCE-MRI对脑进行持续研究,以统计分析群体gd-dtpa pk。我们发现Gd-DTPA(IV 0.025mmol / kg)的PK具有37.3 +/- 6.6分钟的半衰期,并且更好地拟合到比较高剂量的线性T1- [Gd-DTPA]关系(上升到0.1 mmol / kg)。曲线(AUC)下的面积为0.025mmol / kg为337 +/- 0.46,这是0.1mmol / kg的四分之一。在人口分析中,剂量为0.025mmol / kg GD-DTPA,在GD-DTPA的PK中提供了小于5%的对象依赖性变异。通过使用与非线性关系相比具有较低估计误差的线性关系,给予0.025mmol / kg Gd-DTPA的给药0.025mmol / kg gd-dtpa从t1估计[gd-dtpa]。具有四分之一剂量Gd-DTPA的DCE-MRI对检测[GD-DTPA]的变化更敏感。 (c)2016年Elsevier Inc.保留所有权利。

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